Immune responses in a community with a high incidence of tuberculosis
dc.contributor.advisor | Beyers, A. D. | en_ZA |
dc.contributor.advisor | Van Helden, P. D. | en_ZA |
dc.contributor.advisor | Beyers, Nulda | en_ZA |
dc.contributor.author | Adams, Joanita Frances Ann | en_ZA |
dc.contributor.other | Stellenbosch University. Faculty of Medicine & Health Sciences. Dept. of Biomedical Sciences. Molecular Biology and Human Genetics. | en_ZA |
dc.date.accessioned | 2012-08-27T11:33:11Z | |
dc.date.available | 2012-08-27T11:33:11Z | |
dc.date.issued | 2004-03 | en |
dc.description | Thesis (PhD)--Stellenbosch University, 2004 | en_ZA |
dc.description.abstract | ENGLISH ABSTRACT: It is estimated that about one third of the world's population is infected with Mycobacterium tuberculosis (M. tuberculosis). Of those infected, only 10 % will develop disease of which 3-5 % will relapse after completion of treatment. Susceptibility to M tuberculosis or relapse following treatment, may be due to environmental influences such as poverty-related factors including intestinal parasites (helminths), and/or genetic factors, all of which can influence the immune response to M. tuberculosis. In the current study, the epidemiology of mycobacterial infection and helminths was studied in two adjacent suburbs of Cape Town, South Africa. These communities had a tuberculosis notification rate of over 1 000/100 000 population with rampant infestations by helminths such as Ascaris lumbricoides and Trichuris trichiura. M. tuberculosis infection and Bacille Calmette Guerin (BCG) vaccination induce a Thl (type 1) immune response, while a Th2 (type 2) immune response is required for expulsion of intestinal parasites. Type 1 and type 2 responses negatively cross regulate each other in vitro and in experimental models. The interaction of these two immune responses in the study community, were investigated. It was hypothesised that susceptibility to M. tuberculosis and progression to disease may be increased in individuals mounting prominent type 2 immune responses, manifested by high serum IgE levels. Furthermore it is proposed that that poverty-related factors and intestinal parasites, specifically those trafficking through the lungs, could further augment the type 2 dominance in the study community. Results presented show that serum IgE concentrations, surrogate marker for type 2 activation, were high among healthy adults, confirming the dominance of type 2 responses. When characterised in census blocks or enumerator sub-districts (ESDs), IgE levels correlated with the tuberculosis notification rate per ESD. The notification rate of tuberculosis also correlated with the socio-economic status, female literacy and population density of the study population. Although these correlations do not necessarily imply a causal relationship, these factors are associated with susceptibility to M. tuberculosis. It was also shown that IgE concentrations decreased significantly after successful treatment of tuberculosis, showing that IgE concentrations in humans can be down-regulated under these circumstances, presumably due to enhancement of a type 1 response. Furthermore, as a reason for the high serum IgE concentrations in the study population, the helminth burden was subsequently measured in all primary school children in the study community. Results show that more than 50 % of the children recruited were infected with A. lumbricoides and/or T. trichiura. Schools situated in the poorest areas with the highest tuberculosis notification rates, presented with the highest prevalences of helminths. All the children, irrespective of their helminth status or their participation in the study, subsequently received ant-helminthic treatment. The BCG vaccination scar status and Mantoux skin test responses were available on a sub-sample of the above-mentioned school children. Although it is assumed that most children receive BCG vaccination in the neonatal period, only two thirds of the children had evidence of a BCG scar. The results show that the prevalence of BCG scar positivity, while independent of age, was lower in children around 11 years of age. In contrast to the broad constancy of BCG scar expression, the percentage of children showing Mantoux reactivity increased with age, from 13 % at 6 years to 65 % at mid teenage. The time course of Mantoux conversion with age indicated that any tuberculin sensitivity, induced by the BCG, waned within the first few years of life and that PPD responsiveness thereafter was induced by environmental exposure to M. tuberculosis. Contrary to the ThllTh2 paradigm, the prevalence of helminth infection in children with a BCG scar was marginally lower than in those without one. A relatively weak positive correlation was found between tuberculin responsiveness and helminth infection and this correlation was most marked in children without a BCG scar. In this subgroup, children who were infected with helminths were more likely to be PPD responsive than those who were not infected. The data showed that conversion to PPD sensitivity predisposed to helminth infection. The results suggest that the effect of helminth infection on the development of clinical tuberculosis is such that those with large worm burdens and who make good PPD responses are likely to be resistant whereas those who deal very effectively with these parasites and who make weaker PPD responses are more likely to be susceptible. The data also indicate that the BCG vaccine used in this study does not give rise to a latent infection whereas the pathogenic M. tuberculosis does so and repeatedly stimulates an immune response to it. In a separate study, it was demonstrated how the host response to M. tuberculosis differs in patients at risk for developing tuberculosis after successful completion of treatment, compared to those who have protective immunity. Individuals participating in the study were also interviewed to understand their social and economic background and how it relates to the disease. Purified protein derivative (PPD) and M. tuberculosis-induced cytokine responses were determined in the study groups. The results show that single immunological marker of susceptibility could not be distinguished, but rather immunological patterns of susceptibility were observéd. Individuals who have had tuberculosis once before and who had been cured, presented with an immuno-suppressive profile, which included high concentrations of IL-lO, TGF-13 as well as high IgE levels. This type of profile suggests that although these individuals have had tuberculosis once before, they have not acquired protective immunity and would be susceptible to reinfection and progression to disease. Furthermore, the interviews conducted showed that most of the people included in this study were poor, unemployed, undernourished and lived in overcrowded conditions. It seems inevitable that those individuals with the immuno-suppressed profile living in poverty would present with a second episode of tuberculosis in the near future. We conclude that in the study community, which has a typical third world setting, poverty-related factors including helminths, could contribute to a dominant type 2 immune response which in tum, would down-regulate the protective type I response, resulting in an enhanced susceptibility to M. tuberculosis and progression to disease. | en_ZA |
dc.description.abstract | AFRIKAANSE OPSOMMING: Dit word beraam dat ongeveer een derde van die wêreld se populasie geïnfekteer is met Mycobacterium tuberculosis (M. tuberculosis). Van diegene wat wel geïnfekteer is, sal slegs 10 % siekte ontwikkel met 3-5 % wat 'n relaps episode sal ervaar na voltooiing van behandeling. Vatbaarheid vir M. tuberculosis of 'n relaps episode gevolg na behandeling, mag toegeken word aan armoede-verwante faktore wat intestinale parasiete (helminte) asook genetiese faktore, insluit. Hierdie faktore het die vermoë om die immuun respons teen M. tuberculosis te beïnvloed. In die huidige studie, is die epidemiologie van die mikobakteriele infeksie en helminte bestudeer in twee aangrensende voorstede van Kaapstad, Suid Afrika. Hierdie gemeenskappe het 'n tuberkulose aanmeldings koers van 1 000/1 00 000 populasie met verpreide infestasies met helminte soos Ascaris lumbricoides and Trichuris trichiura. Infeksie met M tuberculosis en vaksinasie met Bacille Calmette Guerin (BeG), induseer 'n Th1 (tipe 1) immuun respons, terwyl 'n Th2 immuun respons benodig word vir die eliminasie van intestinale parasiete. Die interaksie tussen die twee immuun response was in die huidige studie populasie bestudeer. Dit word gepostuleer dat persone met 'n sterk tipe 2 immuun respons, gemanifesteer deur hoë serum IgE vlakke, vatbaar is vir infeksie met M. tuberculosis en progressie tot siekte. Verder was dit voorgestel dat armoede-verwante faktore en intestinal parasiete, veral parasiete wat deur die longe beweeg, 'n dominante tipe 2 respons verder kan versterk. Die resultate voorgestel, wys daarop dat serum IgE konsentrasies, 'n surrogaat merker vir tipe 2 aktivering, hoog was in gesonde volwassenenes. Dit het die siening van 'n dominante tipe 2 respons bevestig. IgE vlakke was bereken vir elke sensus blok of enumerator sub-distrik (ESD) en het gekorreleer met die tuberkulose annmeldings koers per ESD. Die aanmeldings koers het ook gekorreleer met die sosio-ekonomiese status, vroulike geletterdheid en populasie digtheid. Alhoewel hierdie korrelasies nie noodwending dui op 'n oorsaak en gevolg verhouding nie, is dit duidelik dat hierdie faktore kan bydra tot vatbaarheid vir M. tuberculosis. Dit was ook getoon dat IgE konsentrasies beduidend afneem na suksesvolle behandeling van tuberkulose. Dit wys daarop dat IgE konsentrasies in mense afgeruleer kan an waarskynlik dui op 'n verhoogde tipe 1 respons. Verder, as 'n rede vir die hoë IgE konsentrasies in die studie populasie, is die helmint ladings gevolglik in alle prim ere skool kinders in die studie populasie, gemeet. Die resultate dui daarop dat meer as 50 % van die kinders ingesluit, geïnfekteer was met A. lumbricoides en/of T. trichiura. Skole in areas met die hoogste armoede syfer en tuberkulose annmeldings koers, het ook die hoogste prevalensie van helminte gehad. Alle kinders, ongeag hulle helmint status of hulle deelname in die studie, het gevolglik anti-helmintiese behandeling ontvang. BeG vaksinasie littekens en Mantoux vel toets response was beskikbaar op 'n subpopulasie van die bogenoemde skool kinders. Alhoewel dit aanvaar word dat die meerderheid van kinders BeG vaksinasie in die neonatale periode ontvang het, het slegs twee derdes van die kinders 'n BeG litteken getoon. Die resulatate dui daarop dat die prevalensie van BeG litteken positiwiteit, onafhanklik van ouderdom, laer was in kinders rondom die ouderdom van 11 jaar. In kontras met die konstante uitdrukking van BeG littekens, het die persentasie van Mantoux reaktiwiteit verhoog met ouderdom vanaf 13 % by 6 jaar tot 65 % teen 15 jarige ouderdom. Die tyd koers van Mantoux omskakeling met ouderdom dui daarop dat tuberkulin sensitiwiteit, geïnduseer deur BeG, afneem binne die eerste paar jaar van lewe en dat PPD responsiwiteit daarna deinduseer word deur omgewings blootstelling aan M. tuberculosis. In kontras met die ThllTh2 paradigma, was die prevalensie van helmint infeksies in kinders met 'n BeG litteken marginaal laer teenoor hulle sonder 'n litteken. 'n Relatiewe swak posititiewe korrelasie was gevind tussen tuberkulin responsiwiteit en helmint infeksie. Hierdie korrelasie was meer beduidend in kinders sonder 'n litteken. In hierdie sub-groep, was die helmintgeïnfekteerde kinders meer geneig om PPD responsief te wees teenoor hulle wat nie geïnfekteer was nie. Die data wys daarop dat omskakeling na PPD sensiwiteit kan lei tot infeksie met helminte. Die resultate stel voor dat die effek van helmint infeksie op die ontwikkeling van kliniese tuberkulose van so 'n aard is dat diegene met groot wurm ladings en wat goeie PPD response toon, meer geneig sal wees om weerstandig te wees. Diegene egter wat die parasiete beter kan beheer and wat goeie PPD response toon, sal meer geneig wees om vatbaar te wees vir tuberkulose. Die data dui ook daarop dat die BeG vaksien wat in die studie gebruik was, nie lei tot latente infeksie nie, terwyl patogene M tuberculosis dit wel doen en herhaardelik die immuun respons sal stimuleer. In 'n aparte studie, was dit gedemonstreer dat die gasheer-respons teen M. tuberculosis in pasiënte wat die gevaar loop om na suksesvolle voltooiing van behandeling, weer tuberkulose te ontwikkel, verskil van diegene wat beskermende immuniteit het. Onderhoude was ook gevoer met indiwidue wat deelgeneem het aan die studie, om ten einde hul sosiale en ekonomiese agtergrond te verstaan en hoe dit gekoppel is aan die siekte. Purified protein derivative (PPD) en M. tuberculosis-geinduseerde sitokien response was in die studie groepe bepaal. Die resultate wys daarop dat alhoewel 'n enkele immunologiese merker nie geidentifiseer kon word nie, was immunologiese patrone vir vatbaarheid welopgemerk. Indiwidue wat reeds een episode van tuberkulose gehad het en suksesvolle behandeling ontvang het, het 'n onderdrukte immuun profiel getoon. Dit het ingesluit hoë vlakke van die sitokiene, IL-lO en TGF-J3 asook hoë vlakke van serum IgE. Hierdie tipe profiel stel voor dat ten spyte van die vorige tuberkulose episode, hierdie persone nie beskermende immunitiet ontwikkel nie en dus vatbaar is vir herinfeksie en progressie tot siekte. Die onderhoude het getoon dat die meerderheid van mense in die studie populasie onder armoedige oorbevolkte omstandighede lewe, wat werkloosheid en ondervoeding insluit. Die studie het verder getoon dat hierdie indiwidue met die onderdrukte immuun profiel en wat in armoede lewe, in die nabye toekoms vatbaar is vir 'n tweede episode van tuberkulose. In die studie gemeenskap, met 'n tipiese derde wêreld opset, is daar gewys dat armoedeverwante faktore en helminte, mag bydra tot 'n dominante tipe 2 immuun respons wat op sy beurt, die beskermende tipe 1 response sal af-reguleer. Dit sal uiteindelik lei tot verhoogde vatbaarheid vir M. tuberculosis en uiteindelik progressie tot siekte (tuberkulose). | af_ZA |
dc.format.extent | 334 p. : ill. | en_ZA |
dc.identifier.uri | http://hdl.handle.net/10019.1/49985 | |
dc.language.iso | en_ZA | |
dc.publisher | Stellenbosch : Stellenbosch University | en_ZA |
dc.rights.holder | Stellenbosch University | en_ZA |
dc.subject | Tuberculosis | en_ZA |
dc.subject | Tuberculosis -- Immunological aspects | en_ZA |
dc.subject | Dissertations -- Medicine | en_ZA |
dc.title | Immune responses in a community with a high incidence of tuberculosis | en_ZA |
dc.type | Thesis | en_ZA |
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